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Long-lasting T cell responses to biological warfare Vaccines in human vaccinees

机译:T细胞对人类疫苗中生物战疫苗的持久反应

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摘要

Background. Medical countermeasures against biological warfare include the use of vaccines for anthrax and plague, which require repeated dosing and adjuvant to achieve adequate protection from threats such as inhalational anthrax and pneumonic plague. Despite the widespread use of these measures in preparation for recent military deployments, little is known about the cell-mediated immune response that is induced by these vaccines, in comparison with conventional vaccines, such as pertussis or tetanus-diphtheria vaccines. Methods. To examine this question, we used cytokine enzyme-linked immunospot assays to measure interferon-gamma, interleukin ( IL)-2, IL-4, and IL-13-producing cells in military service personnel vaccinated during the Gulf War of 1990-1991. Results. Our data indicate that 12-15 years after vaccination against anthrax and plague, antigen-specific T cell recall responses are present in the circulation and are comparable in magnitude to those for tetanus-diphtheria toxoids. Recall responses to anthrax were an approximately equal mixture of type 1 T helper cell ( interferon-gamma and IL-2) and type 2 T helper cell ( predominantly IL-13) responses, whereas plague cellular immunity was more polarized toward type 1 T helper cell responses. Responder cell frequency and type were similar to that against conventional tetanus-diphtheria ( mixed type 1 and type 2 T helper cells) vaccine. When veterans were divided according to whether or not they reported multisymptom-illness, there was no difference in the frequency or type of cellular response, although the number of cases in each group was small, and these data should be interpreted as preliminary. Conclusions. This study shows that, despite any putative limitations of vaccines for anthrax and plague in terms of achieving protective host immunity, long-lasting cell-mediated responses are generated with these agents
机译:背景。对抗生物战的医学对策包括使用炭疽和鼠疫疫苗,这些疫苗需要反复给药和佐剂才能获得对吸入性炭疽和肺鼠疫等威胁的充分保护。尽管这些措施广泛用于最近的军事部署,但与常规疫苗(如百日咳或破伤风-白喉疫苗)相比,由这些疫苗诱导的细胞介导的免疫反应知之甚少。方法。为了检查这个问题,我们使用了细胞因子酶联免疫斑点测定法来测量1990-1991年海湾战争期间接种疫苗的军人的干扰素-γ,白介素(IL)-2,IL-4和IL-13产生细胞。结果。我们的数据表明,针对炭疽和鼠疫疫苗接种后的12-15年,循环中存在抗原特异性T细胞召回反应,其强度与破伤风-白喉类毒素相当。召回对炭疽的反应大约是1型T辅助细胞(干扰素-γ和IL-2)和2型T辅助细胞(主要是IL-13)反应的混合物,而瘟疫细胞免疫力更偏向于1型T辅助细胞细胞反应。应答细胞的频率和类型与常规破伤风-白喉(混合的1型和2型T辅助细胞)疫苗相似。根据是否报告多症状疾病对退伍军人进行划分时,尽管每组中的病例数很少,但细胞反应的频率或类型没有差异,这些数据应被解释为初步数据。结论。这项研究表明,尽管炭疽和鼠疫疫苗在实现保护性宿主免疫方面有任何假定的局限性,但这些试剂仍能产生持久的细胞介导的反应

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